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Discovery of N-aryl-2-acylindole human glucagon receptor antagonists |
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| Authors: | Sinz Christopher Bittner Amy Brady Ed Candelore Mari Dallas-Yang Qing Ding Victor Jiang Guoqiang Lin Zhen Qureshi Sajjad Salituro Gino Saperstein Richard Shang Jackie Szalkowski Deborah Tota Laurie Vincent Stella Wright Michael Xu Shiyao Yang Xiaodong Zhang Bei Tata James Kim Ronald Parmee Emma R |
| Institution: | Discovery and Preclinical Sciences, Merck Research Laboratories, Rahway, NJ 07065, USA. christopher_sinz@merck.com |
| Abstract: | A novel class of N-aryl-2-acylindole human glucagon receptor (hGCGR) antagonists is reported. These compounds demonstrate good pharmacokinetic profiles in multiple preclinical species. One compound from this series, indole 33, is orally active in a transgenic murine pharmacodynamic model. Furthermore, a 1mg/kg oral dose of indole 33 lowers ambient glucose levels in an ob/ob/hGCGR transgenic murine diabetes model. This compound was deemed suitable for preclinical safety studies and was found to be well tolerated in an 8-day experimental rodent tolerability study. The combination of preclinical efficacy and safety observed with compound 33 highlights the potential of this class as a treatment for type 2 diabetes. |
| Keywords: | Glucagon Diabetes Glucose Antagonist Indole |
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